Common genetic variation and susceptibility to partial epilepsies: A genome-wide association study
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Kasperavi-iüte, D. Catarino, C.B. Heinzen, E.L. Depondt, C. Cavalleri, G.L. Caboclo, L.O. Tate, S.K. Jamnadas-Khoda, J. Chinthapalli, K. Clayton, L.M.S. Shianna, K.V. Radtke, R.A. Mikati, M.A. Gallentine, W.B. Husain, A.M. Alhusaini, S. Leppert, D. Middleton, L.T. Gibson, R.A. Johnson, M.R. Matthews, P.M. Hosford, D. Heuser, K. Amos, L. Ortega, M. Zumsteg, D. Wieser, H.-G. Steinhoff, B.J. Krämer, G. Hansen, J. Dorn, T. Kantanen, A.-M. Gjerstad, L. Peuralinna, T. Hernandez, D.G. Eriksson, K.J. Kälviäinen, R.K. Doherty, C.P. Wood, N.W. Pandolfo, M. Duncan, J.S. Sander, J.W. Delanty, N. Goldstein, D.B. Sisodiya, S.M., Common genetic variation and susceptibility to partial epilepsies: A genome-wide association study, Brain, 133, 7, 2010, 2136 - 2147
Abstract
Partial epilepsies have a substantial heritability. However, the actual genetic causes are largely unknown. In contrast to many
other common diseases for which genetic association-studies have successfully revealed common variants associated with
disease risk, the role of common variation in partial epilepsies has not yet been explored in a well-powered study. We under-
took a genome-wide association-study to identify common variants which influence risk for epilepsy shared amongst partial
epilepsy syndromes, in 3445 patients and 6935 controls of European ancestry. We did not identify any genome-wide significant
association. A few single nucleotide polymorphisms may warrant further investigation. We exclude common genetic variants
with effect sizes above a modest 1.3 odds ratio for a single variant as contributors to genetic susceptibility shared across the
partial epilepsies. We show that, at best, common genetic variation can only have a modest role in predisposition to the partial
epilepsies when considered across syndromes in Europeans. The genetic architecture of the partial epilepsies is likely to be very
complex, reflecting genotypic and phenotypic heterogeneity. Larger meta-analyses are required to identify variants of smaller
effect sizes (odds ratio
5
1.3) or syndrome-specific variants. Further, our results suggest research efforts should also be directed
towards identifying the multiple rare variants likely to account for at least part of the heritability of the partial epilepsies. Data
emerging from genome-wide association-studies will be valuable during the next serious challenge of interpreting all the
genetic variation emerging from whole-genome sequencing studies
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Sponsor: Science Foundation Ireland (SFI)
Grant Number: 08/RFP/GEN1538
Author's Homepage: http://people.tcd.ie/cdohert
Type of material: Journal Article

